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RU2017126598A - RNA AGENTS FOR GST-PI GENE MODULATION - Google Patents

RNA AGENTS FOR GST-PI GENE MODULATION Download PDF

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RU2017126598A
RU2017126598A RU2017126598A RU2017126598A RU2017126598A RU 2017126598 A RU2017126598 A RU 2017126598A RU 2017126598 A RU2017126598 A RU 2017126598A RU 2017126598 A RU2017126598 A RU 2017126598A RU 2017126598 A RU2017126598 A RU 2017126598A
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nucleic acid
cancer
acid molecule
seq
molecule according
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RU2017126598A
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Венбин ИН
Кендзироу МИНОМИ
Йенс ХАРБОРТ
Хирокадзу ТАКАХАСИ
Эрика ТЕРАДА
Дзун ЧЖАН
Мохаммад АХМАДИАН
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Нитто Денко Корпорейшн
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Claims (27)

1. Молекула нуклеиновой кислоты, где:1. The nucleic acid molecule, where: молекула имеет полинуклеотидную смысловую цепь и полинуклеотидную антисмысловую цепь;the molecule has a polynucleotide sense strand and a polynucleotide antisense strand; каждая цепь молекулы имеет длину от 15 до 30 нуклеотидов;each chain of the molecule has a length of 15 to 30 nucleotides; непрерывная область от 15 до 30 нуклеотидов антисмысловой цепи комплементарна последовательности мРНК, кодирующей GST-π;a continuous region of 15 to 30 nucleotides of the antisense strand is complementary to the mRNA sequence encoding GST-π; по меньшей мере, часть смысловой цепи комплементарна, по меньшей мере, части антисмысловой цепи, и молекула имеет дуплексную область длиной от 15 до 30 нуклеотидов.at least a part of the sense strand is complementary to at least a part of the antisense strand, and the molecule has a duplex region of 15 to 30 nucleotides in length. 2. Молекула нуклеиновой кислоты по п.1, отличающаяся тем, что антисмысловая цепь представляет собой SEQ ID NO: 1341, а смысловая цепь представляет собой SEQ ID NO: 1276 или их химически модифицированные цепи.2. The nucleic acid molecule according to claim 1, characterized in that the antisense chain is SEQ ID NO: 1341, and the sense strand is SEQ ID NO: 1276 or their chemically modified chains. 3. Молекула нуклеиновой кислоты по п.1, отличающаяся тем, что антисмысловая цепь представляет собой SEQ ID NO: 1305, а смысловая цепь представляет собой SEQ ID NO: 1240 или их химически модифицированные цепи.3. The nucleic acid molecule according to claim 1, characterized in that the antisense chain is SEQ ID NO: 1305, and the sense strand is SEQ ID NO: 1240 or their chemically modified chains. 4. Молекула нуклеиновой кислоты по п.1, отличающаяся тем, что непрерывная область антисмысловой цепи длиной от 15 до 30 нуклеотидов, которая комплементарна последовательности мРНК, кодирующей GST-π, расположена в дуплексной области молекулы.4. The nucleic acid molecule according to claim 1, characterized in that the continuous region of the antisense strand is from 15 to 30 nucleotides in length, which is complementary to the mRNA sequence encoding GST-π, located in the duplex region of the molecule. 5. Молекула нуклеиновой кислоты по п.1, отличающаяся тем, что непрерывную область антисмысловой цепи длиной от 15 до 30 нуклеотидов, которая комплементарна последовательности мРНК, кодирующей GST-π, выбирают из последовательности человеческого GSTP1, где мРНК человеческого GSTP1 представляет собой SEQ ID NO: 1.5. The nucleic acid molecule according to claim 1, characterized in that the continuous region of the antisense strand from 15 to 30 nucleotides in length, which is complementary to the mRNA sequence encoding GST-π, is selected from the sequence of human GSTP1, where the human GSTP1 mRNA is SEQ ID NO : one. 6. Молекула нуклеиновой кислоты по п.1, отличающаяся тем, что последовательность мРНК, кодирующую GST-π, выбирают из группы, состоящей из 5'UTR-положений 1-249 SEQ ID NO: 1, CDS-положений 250-882 SEQ ID NO: 1, и 3'UTR положений 883-986 SEQ ID NO: 1.6. The nucleic acid molecule according to claim 1, characterized in that the mRNA sequence encoding GST-π is selected from the group consisting of 5'UTR positions 1-249 SEQ ID NO: 1, CDS positions 250-882 SEQ ID NO: 1, and 3'UTR positions 883-986 of SEQ ID NO: 1. 7. Молекула нуклеиновой кислоты по п.1, отличающаяся тем, что антисмысловая цепь содержит последовательность, выбранную из любой из SEQ ID NO: 609-1215.7. The nucleic acid molecule according to claim 1, characterized in that the antisense chain contains a sequence selected from any of SEQ ID NO: 609-1215. 8. Молекула нуклеиновой кислоты по п.1, отличающаяся тем, что антисмысловая цепь содержит последовательность, выбранную из любой из SEQ ID NO: 1281-1345.8. The nucleic acid molecule according to claim 1, characterized in that the antisense chain contains a sequence selected from any of SEQ ID NO: 1281-1345. 9. Молекула нуклеиновой кислоты по п.1, отличающаяся тем, что молекула состоит из пары антисмысловой и смысловой цепи, выбранной из группы, состоящей из SEQ ID NO: 1240 и 1305, SEQ ID NO: 1265 и 1330, SEQ ID NO: 1267 и 1332, SEQ ID NO: 1269 и 1334 и SEQ ID NO: 1276 и 1341.9. The nucleic acid molecule according to claim 1, characterized in that the molecule consists of a pair of antisense and sense strands selected from the group consisting of SEQ ID NO: 1240 and 1305, SEQ ID NO: 1265 and 1330, SEQ ID NO: 1267 and 1332, SEQ ID NO: 1269 and 1334 and SEQ ID NO: 1276 and 1341. 10. Молекула нуклеиновой кислоты по п.1, отличающаяся тем, что каждая цепь молекулы имеет длину от 18 до 22 нуклеотидов.10. The nucleic acid molecule according to claim 1, characterized in that each chain of the molecule has a length of from 18 to 22 nucleotides. 11. Молекула нуклеиновой кислоты по п.1, отличающаяся тем, что дуплексная область имеет длину 19 нуклеотидов.11. The nucleic acid molecule according to claim 1, characterized in that the duplex region has a length of 19 nucleotides. 12. Молекула нуклеиновой кислоты по п.1, отличающаяся тем, что полинуклеотидная смысловая цепь и полинуклеотидная антисмысловая цепь соединены в виде одной цепи и образуют дуплексную область, соединенную на одном конце петлей.12. The nucleic acid molecule according to claim 1, characterized in that the polynucleotide sense strand and the polynucleotide antisense strand are connected as a single strand and form a duplex region connected at one end of the loop. 13. Молекула нуклеиновой кислоты по п.1, отличающаяся тем, что молекула имеет тупой конец.13. The nucleic acid molecule according to claim 1, characterized in that the molecule has a blunt end. 14. Молекула нуклеиновой кислоты по п.1, отличающаяся тем, что молекула имеет один или несколько 3'-выступающих участков.14. The nucleic acid molecule according to claim 1, characterized in that the molecule has one or more 3'-protruding sections. 15. Молекула нуклеиновой кислоты по п.1, отличающаяся тем, что молекула представляет собой молекулу РНКи, активную для сайленсинга генов.15. The nucleic acid molecule according to claim 1, characterized in that the molecule is an RNAi molecule that is active for gene silencing. 16. Молекула нуклеиновой кислоты по п.1, отличающаяся тем, что молекула представляет собой дцРНК, киРНК, микро-РНК или кшРНК, активную для сайленсинга генов.16. The nucleic acid molecule according to claim 1, characterized in that the molecule is dsRNA, siRNA, micro-RNA or kshRNA, active for gene silencing. 17. Молекула нуклеиновой кислоты по п.1, отличающаяся тем, что молекула активна для ингибирования экспрессии GST-π.17. The nucleic acid molecule according to claim 1, characterized in that the molecule is active for inhibiting the expression of GST-π. 18. Молекула нуклеиновой кислоты по п.1, отличающаяся тем, что молекула имеет IC50 для нокдауна GST-π менее чем 100 пМ.18. The nucleic acid molecule according to claim 1, characterized in that the molecule has an IC50 for GST-π knockdown of less than 100 pM. 19. Композиция, содержащая одну или несколько молекул нуклеиновой кислоты по любому из пп.1-18 и фармацевтически приемлемый носитель.19. A composition comprising one or more nucleic acid molecules according to any one of claims 1 to 18 and a pharmaceutically acceptable carrier. 20. Композиция по п.19, отличающаяся тем, что носитель представляет собой липидную молекулу или липосому.20. The composition according to claim 19, characterized in that the carrier is a lipid molecule or liposome. 21. Способ лечения заболевания, ассоциированного с экспрессией GST-π, причем способ включает введение композиции по п.19 объекту, нуждающемуся в этом.21. A method of treating a disease associated with the expression of GST-π, the method comprising administering a composition according to claim 19 to an object in need thereof. 22. Способ по п.21, отличающийся тем, что заболевание представляет собой злокачественную опухоль.22. The method according to item 21, wherein the disease is a malignant tumor. 23. Способ по п.22, отличающийся тем, что злокачественная опухоль присутствует в заболевании, выбранном из группы, состоящей из злокачественных опухолей, связанных с экспрессией GST, злокачественных опухолей, вызванных клетками, экспрессирующими мутантный KRAS, саркомы, фибросаркомы, злокачественной фиброзной гистиоцитомы, липосаркомы, рабдомиосаркомы, лейомиосаркомы, ангиосаркомы, саркомы Капоши, лимфангиосаркомы, синовиальной саркомы, хондросаркомы, остеосаркомы, карциномы, опухоли головного мозга, рака головы и шеи, рака молочной железы, рака легких, рака пищевода, рака желудка, рака прямой кишки, колоректального рака, рака толстой кишки, рака печени, рака поджелудочной железы, рака желчного пузыря, рака желчных протоков, рака почек, уретрального рака, рака мочевого пузыря, рака предстательной железы, рака яичек, рака полового члена, рака матки, рака яичников, рака кожи, рака кости, лейкоза, злокачественной лимфомы, эпителиальных злокачественных опухолей и неэпителиальных злокачественных опухолей.23. The method according to item 22, wherein the malignant tumor is present in a disease selected from the group consisting of malignant tumors associated with the expression of GST, malignant tumors caused by cells expressing mutant KRAS, sarcomas, fibrosarcoma, malignant fibrous histiocytoma, liposarcoma, rhabdomyosarcoma, leiomyosarcoma, angiosarcoma, Kaposi’s sarcoma, lymphangiosarcoma, synovial sarcoma, chondrosarcoma, osteosarcoma, carcinoma, brain tumor, head and neck cancer, breast cancer, aka lung, cancer of the esophagus, stomach cancer, colon cancer, colorectal cancer, colon cancer, liver cancer, pancreatic cancer, gall bladder cancer, bile duct cancer, kidney cancer, urethral cancer, bladder cancer, prostate cancer, cancer testicles, penile cancer, uterine cancer, ovarian cancer, skin cancer, bone cancer, leukemia, malignant lymphoma, epithelial malignancies and non-epithelial malignancies.
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